6533b7d2fe1ef96bd125eac7

RESEARCH PRODUCT

MYC-driven epigenetic reprogramming favors the onset of tumorigensis by inducing a stem cell-like state

Vittoria PoliMatilde TodaroSilvano BosariAlice TurdoAnnarita MiluzioValentina VairaMiriam GaggianesiAlessandro CherubiniSara FerrilloAlessio ZippoAurora ChinniciGabriella GaudiosoAlessandra FascianiSilvio BicciatoElisa LipariLuca FagnocchiStefania Mazzoleni

subject

medicine.anatomical_structureCell of originCellmedicineTumor initiationEpigeneticsBiologyStem cellEnhancerTranscription factorReprogrammingCell biology

description

AbstractBreast cancer consists of highly heterogeneous tumors, whose cell of origin and driver oncogenes resulted difficult to be uniquely defined. Here we report that MYC acts as tumor reprogramming factor in mammary epithelial cells by inducing an alternative epigenetic program, which triggers loss of cell identity and activation of oncogenic pathways. Over-expression of MYC induces transcriptional repression of lineage-specifying transcription factors, causing decommissioning of luminal-specific enhancers. MYC-driven dedifferentiation supports the onset of a stem cell-like state by inducing the activation of de novo enhancers, which drive the transcriptional activation of oncogenic pathways. Furthermore, we demonstrate that the MYC-driven epigenetic reprogramming favors the formation and maintenance of tumor initiating cells endowed with metastatic capacity. This study supports the notion that MYC-driven tumor initiation relies on cell reprogramming, which is mediated by the activation of MYC-dependent oncogenic enhancers, thus establishing a therapeutic rational for treating basal-like breast cancers.

yearjournalcountryeditionlanguage
2017-12-29
https://doi.org/10.1101/241042